2016
DOI: 10.1016/j.virusres.2016.01.012
|View full text |Cite
|
Sign up to set email alerts
|

Two second-site mutations compensate the engineered mutation of R7A in vesicular stomatitis virus nucleocapsid protein

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
3

Citation Types

0
3
0

Year Published

2019
2019
2020
2020

Publication Types

Select...
2
2

Relationship

0
4

Authors

Journals

citations
Cited by 4 publications
(3 citation statements)
references
References 24 publications
0
3
0
Order By: Relevance
“…But these VSVs have high cytotoxicity that can lead to rapid death of mice, which limits long-term structural observation and gene manipulation or function research, restricting their applications in neuroscience [23]. Several mutants have been obtained by mutating the N gene related to the replication of VSV [24][25][26][27]. After mutating the seventh amino acid of the N protein (VSV-N R7A ), the replication speed of the virus decreased by 2-3 orders of magnitude within 24 h [24,25], which might be used as a better tracer, but whether it still has the ability of anterograde trans-synaptic labeling is still unknown.…”
Section: Introductionmentioning
confidence: 99%
“…But these VSVs have high cytotoxicity that can lead to rapid death of mice, which limits long-term structural observation and gene manipulation or function research, restricting their applications in neuroscience [23]. Several mutants have been obtained by mutating the N gene related to the replication of VSV [24][25][26][27]. After mutating the seventh amino acid of the N protein (VSV-N R7A ), the replication speed of the virus decreased by 2-3 orders of magnitude within 24 h [24,25], which might be used as a better tracer, but whether it still has the ability of anterograde trans-synaptic labeling is still unknown.…”
Section: Introductionmentioning
confidence: 99%
“…But these VSVs have high cytotoxicity that can lead to rapid death of mice, which limits long-term structural observation and gene manipulation or function research, restricting their applications in neuroscience [23]. Several mutants have been obtained by mutating the N gene related to the replication of VSV [24][25][26][27]. After mutating the seventh amino acid of the N protein (VSV-N R7A ), the replication speed of the virus decreased by 2-3 orders of magnitude within 24 hours [24,25], which might be used as a better tracer, but whether it still has the ability of anterograde trans-synaptic labeling is still unknown.…”
Section: Introductionmentioning
confidence: 99%
“…But these VSVs have high cytotoxicity that can lead to rapid death of mice, which limits long-term structural observation and gene manipulation or function research, restricting their applications in neuroscience [23]. Several mutants have been obtained by mutating the N gene related to the replication of VSV [24][25][26][27]. After mutating the seventh amino acid of the N protein (VSV-N R7A ), the replication speed of the virus decreased by 2-3 orders of magnitude within 24 hours [24,25], which might be used as a better tracer, but whether it still has the ability of anterograde transsynaptic labeling is still unknown.…”
Section: Introductionmentioning
confidence: 99%